Melatonin inhibits colon cancer RKO cell migration by downregulating Rho-associated protein kinase expression via the p38/MAPK signaling pathway

Liu, Zhen; Zou, Duobing; Yang, Xiaoping; Xue, Xiaolong; Zuo, Li; Zhou, Qing; Hu, Ruolei; Wang, Yuan

doi:10.3892/mmr.2017.7836

Cited by 34 publications

(23 citation statements)

References 36 publications

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“…Moreover, melatonin prevented the cytoskeletal disorganization of RKO cells, thereby inhibiting cell migration. Accordingly, the membrane expression of TJ‐structural proteins occludin and ZO‐1 has been reported upregulated on cell surface of RKO cells treated with melatonin (2.5 mM, up to 48 hours), thus inhibiting their migration and restraining their metastatic dissemination . Similar findings have been recently documented in human gastric carcinoma cells, in which millimolar melatonin (10 −4 M, 48 hours) relocated and concentrate occludin and ZO‐1 on their cell surface, thereby enhancing adhesion and inhibiting their migration and metastasis capacity .…”

Section: Multimodal Approach Using Melatonin Against Progression and supporting

confidence: 73%

“…Accordingly, the membrane expression of TJ-structural proteins occludin and ZO-1 has been reported upregulated on cell surface of RKO cells treated with melatonin (2.5 mM, up to 48 hours), thus inhibiting their migration and restraining their metastatic dissemination. 241 Similar findings have been recently documented in human gastric carcinoma cells, in which millimolar melatonin (10 −4 M, 48 hours) relocated and concentrate occludin and ZO-1 on their cell surface, thereby enhancing adhesion and inhibiting their migration and metastasis capacity. 124 Despite this, the mechanistic underlying the ability of melatonin to modulate TJ's functionality and inhibiting the invasive capacity of tumor cells from CRC and other neoplasias has been sparsely investigated and, consequently, a lot of work remains to be done.…”

supporting

confidence: 82%

“…In addition, the analysis of tumor propagation in an athymic nude mouse model has clearly shown that the combination of melatonin (25 mg/kg) and 5‐FU (20 mg/kg) potentiates the growth inhibition of xenografted CRC tumors with respect to that achieved with 5‐FU alone . Moreover, the p38 MAPK signaling, involved in CRC growth and resistance to 5‐FU and other chemotherapies, is downregulated along with the reinforcement of TJ proteins, in RKO colon cancer cells after treatment with 2.5 mM melatonin, as previously discussed regarding the effect of melatonin on the metastatic spreadout of CRC …”

Section: Synergistic Actions Of Melatonin As Adjuvant Treatment In Crcsupporting

confidence: 52%

“…318 Moreover, the p38 MAPK signaling, involved in CRC growth and resistance to 5-FU and other chemotherapies, 354 is downregulated along with the reinforcement of TJ proteins, in RKO colon cancer cells after treatment with 2.5 mM melatonin, as previously discussed regarding the effect of melatonin on the metastatic spreadout of CRC. 241 Even though the above summarized evidence proved that melatonin, per se or as a complementary adjunctive defense against CRC chemotherapy toxicity, is beneficial for relieving CRC patients from adverse side effects of therapeutic regimens, the oncostatic processes by which its works are far from being understood. Thus, for example, there is no unequivocal experimental basis to determine if the therapeutic synergy of melatonin combined with conventional chemotherapy drugs is due to its ability to enhance the oncostatic capacity of the chemotherapeutic agents, or vice versa (drugs amplifying the biological effectivity of melatonin).…”

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confidence: 99%

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The emergence of melatonin in oncology: Focus on colorectal cancer

Gil‐Martín

Egea

Reíter

et al. 2019

Medicinal Research Reviews

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Within the last few decades, melatonin has increasingly emerged in clinical oncology as a naturally occurring bioactive molecule with substantial anticancer properties and a pharmacological profile optimal for joining the currently available pharmacopeia. In addition, extensive experimental data shows that this chronobiotic agent exerts oncostatic effects throughout all stages of tumor growth, from initial cell transformation to mitigation of malignant progression and metastasis; additionally, melatonin alleviates the side effects and improves the welfare of radio/chemotherapy‐treated patients. Thus, the support of clinicians and oncologists for the use of melatonin in both the treatment and proactive prevention of cancer is gaining strength. Because of its epidemiological importance and symptomatic debut in advanced stages of difficult clinical management, colorectal cancer (CRC) is a preferential target for testing new therapies. In this regard, the development of effective forms of clinical intervention for the improvement of CRC outcome, specifically metastatic CRC, is urgent. At the same time, the need to reduce the costs of conventional anti‐CRC therapy results is also imperative. In light of this status quo, the therapeutic potential of melatonin, and the direct and indirect critical processes of CRC malignancy it modulates, have aroused much interest. To illuminate the imminent future on CRC research, we focused our attention on the molecular mechanisms underlying the multiple oncostatic actions displayed by melatonin in the onset and evolution of CRC and summarized epidemiological evidence, as well as in vitro, in vivo and clinical findings that support the broadly protective potential demonstrated by melatonin.

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Section: Multimodal Approach Using Melatonin Against Progression and supporting

confidence: 73%

supporting

confidence: 82%

Section: Synergistic Actions Of Melatonin As Adjuvant Treatment In Crcsupporting

confidence: 52%

mentioning

confidence: 99%

See 2 more Smart Citations

The emergence of melatonin in oncology: Focus on colorectal cancer

Gil‐Martín

Egea

Reíter

et al. 2019

Medicinal Research Reviews

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“…The anticancer efficiency of melatonin has also been investigated over the past two decades . Melatonin has been reported to exert an anti‐proliferative and cytotoxic effect on prostate cancer and suppress cell migration and metastasis in colon cancer and lung cancer . Melatonin plays an important role in the anti‐proliferation of female reproductive cancers.…”

Section: Introductionmentioning

confidence: 99%

Melatonin activates cell death programs for the suppression of uterine leiomyoma cell proliferation

Lin

Tung

Chen

et al. 2019

Journal of Pineal Research

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The circadian nature of melatonin has a protective effect on the progression of female reproductive cancers, including breast and ovarian cancers. However, the effect of melatonin on the growth of uterine leiomyoma is still unclear. In this study, we found that the growth of uterine leiomyoma ELT3 cells was reduced by treatment with melatonin. Treatment with melatonin increased the distribution of sub-G1 phase and increased DNA condensation in ELT3 cells. Melatonin-induced apoptosis and autophagy cell death progression were observed in ELT3 cells. Melatonin exerts a highly selective effect on primary normal human uterine smooth muscle (UtSMC) cells. The UtSMC cell cycle was arrested by melatonin treatment through up-regulation of p21, p27, and PTEN protein expression, but melatonin did not further promote apoptosis program activation. Melatonin reduced cell proliferation in ELT3 cells underlying the activation of melatonin MT1 and MT2 receptors, which in turn down-regulated the Akt-ERK1/2-NFκB signaling pathway. Melatonin reduced ELT3 tumor growth in both xenograft and orthotopic uterine tumor mice models. The extracellular matrix of the tumor was also reduced by melatonin treatment. Taken together, these results suggest that melatonin potentially plays a role in suppression of uterine leiomyoma growth. K E Y W O R D S apoptosis, autophagy, cell cycle, melatonin, uterine leiomyoma (fibroid), uterine smooth muscle cells

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Melatonin as a potential inhibitor of colorectal cancer: Molecular mechanisms

Shafabakhsh

Reíter

Davoodabadi

et al. 2019

J of Cellular Biochemistry

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Colorectal cancer (CRC) is a prevalent disease and a major cause of mortality in the world. Several factors including population aging, poor dietary habits, obesity, insufficient physical activity, and smoking can explain its increased prevalence. CRC is a heterogeneous disease both histopathologically and in term of its molecular and genetic aspects.Melatonin a derivative of tryptophan, is synthesized and released from pineal gland but it is also found in numerous extrapineal tissues including retina, testes, lymphocytes, Harderian gland, gastrointestinal tract, etc. This molecule has several tasks which enhance physiological functions such as antioxidant, antiaging, immunomodulatory, and tumor inhibition.Multiple immunocytochemical studies reported melatonin in the intestinal mucosa where its concentration is greater than in the blood. These findings suggest that melatonin may have a potential inhibitory role in CRC progression. The purpose of this review is to examine the effects of melatonin in molecular pathogenesis and signaling pathways of CRC. K E Y W O R D Scolorectal cancer, modification, pathogenesis, signaling pathways

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Melatonin inhibits colon cancer RKO cell migration by downregulating Rho-associated protein kinase expression via the p38/MAPK signaling pathway

Cited by 34 publications

References 36 publications

The emergence of melatonin in oncology: Focus on colorectal cancer

The emergence of melatonin in oncology: Focus on colorectal cancer

Melatonin activates cell death programs for the suppression of uterine leiomyoma cell proliferation

Melatonin as a potential inhibitor of colorectal cancer: Molecular mechanisms

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